Measurements of Functional Responses in Human Primary Lung Cells as a Basis for Personalized Therapy for Cystic Fibrosis.

Fecha de publicación: 01/02/2015

Autores de IIS La Fe

Amparo Solé Jover

Autor
Juan Pastor Guillem

Autor

Participantes ajenos a IIS La Fe

Awatade, NT
Uliyakina, I
Farinha, C
Clarke, LA
Mendes, K
Ramos, MM
Amaral, MD

Grupos

Infección Grave

Investigador Principal

María Ángeles Tormo Mas

Abstract

BACKGROUND: The best investigational drug to treat cystic fibrosis (CF) patients with the most common CF-causing mutation (F508del) is VX-809 (lumacaftor) which recently succeeded in Phase III clinical trial in combination with ivacaftor. This corrector rescues F508del-CFTR from its abnormal intracellular localization to the cell surface, a traffic defect shared by all Class II CFTR mutants. Our goal here is to test the efficacy of lumacaftor in other Class II mutants in primary human bronchial epithelial (HBE) cells derived from CF patients. METHODS: The effect of lumacaftor was investigated in primary HBE cells from non-CF and CF patients with F508del/F508del, A561E/A561E, N1303K/G542X, F508del/G542X and F508del/Y1092X genotypes by measurements of Forskolin plus Genistein-inducible equivalent short-circuit current (Ieq-SC-Fsk + Gen) in perfused open-circuit Ussing chambers. Efficacy of corrector C18 was also assessed on A561E/A561E and F508del/F508del cells. RESULTS: Our data indicate that A561E (when present in both alleles) responds positively to lumacaftor treatment at equivalent efficacy of F508del in primary HBE cells. Similarly, lumacaftor has a positive impact on Y1092X, but not on N1303K. Our data also show that cells with only one copy of F508del-CFTR respond less to VX-809. Moreover, there is great variability in lumacaftor responses among F508del-homozygous cells from different donors. Compound C18 failed to rescue A561E-CFTR but not in F508del-CFTR, thus plausibly it has a different mechanism of action distinct from lumacaftor. CONCLUSIONS: CF patients with A561E (and likely also those with Y1029X) can potentially benefit from lumacaftor. Moreover, the methodology used here exemplifies how ex vivo approaches may apply personalized therapies to CF and possibly other respiratory diseases.

Datos de la publicación

ISSN/ISSNe:: 2352-3964, 2352-3964
Tipo:: Article
Páginas:: 147-153
DOI:: 10.1016/j.ebiom.2014.12.005
PubMed:: 26137539
Factor de Impacto:: 1,352 SCImago ℠
Cuartil:: Q1 SCImago ℠

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Métricas

Filiaciones

Awatade, NT:: Univ Lisbon, Fac Sci, BioFIG Ctr Biodivers Funct & Integrat Genom, C8 Bdg, P-1749016 Lisbon, Portugal
Uliyakina, I:: Univ Lisbon, Fac Sci, BioFIG Ctr Biodivers Funct & Integrat Genom, C8 Bdg, P-1749016 Lisbon, Portugal
Farinha, C:: Univ Lisbon, Fac Sci, BioFIG Ctr Biodivers Funct & Integrat Genom, C8 Bdg, P-1749016 Lisbon, Portugal
Clarke, LA:: Univ Lisbon, Fac Sci, BioFIG Ctr Biodivers Funct & Integrat Genom, C8 Bdg, P-1749016 Lisbon, Portugal
Mendes, K:: Univ Lisbon, Fac Sci, BioFIG Ctr Biodivers Funct & Integrat Genom, C8 Bdg, P-1749016 Lisbon, Portugal
Sole, A:: Univ Hosp la Fe, Adult Cyst Fibrosis Unit, Valencia 46026, Spain
Pastor, J:: Univ Hosp la Fe, Thorac Surg Serv, Valencia 46009, Spain
Ramos, MM:: Univ Lisbon, Fac Sci, BioFIG Ctr Biodivers Funct & Integrat Genom, C8 Bdg, P-1749016 Lisbon, Portugal
Amaral, MD:: Univ Lisbon, Fac Sci, BioFIG Ctr Biodivers Funct & Integrat Genom, C8 Bdg, P-1749016 Lisbon, Portugal

Keywords

(DeltaIeq-sc), equivalent short-circuit currents; CF, cystic fibrosis; CFTR, cystic fibrosis transmembrane conductance regulator; ENaC, epithelial Na+ channel; Fsk, forskolin; Gen, Genistein; HBE (cells), human bronchial epithelial cells; Innovative treatments; Mutation-specific therapies; Personalized medicine; Rare diseases; Rte, transepithelial resistance.; SEM, standard error of the mean; TEER, transepithelial electrical resistance; Vte, transepithelial voltage